iPSCs as a groundbreaking tool for the study of adverse drug reactions: A new avenue for personalized therapy.

IF 4.6 3区 医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL WIREs Mechanisms of Disease Pub Date : 2024-01-01 Epub Date: 2023-09-28 DOI:10.1002/wsbm.1630
Paola Rispoli, Tatiana Scandiuzzi Piovesan, Giuliana Decorti, Gabriele Stocco, Marianna Lucafò
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Abstract

Induced pluripotent stem cells (iPSCs), obtained by reprogramming different somatic cell types, represent a promising tool for the study of drug toxicities, especially in the context of personalized medicine. Indeed, these cells retain the same genetic heritage of the donor, allowing the development of personalized models. In addition, they represent a useful tool for the study of adverse drug reactions (ADRs) in special populations, such as pediatric patients, which are often poorly represented in clinical trials due to ethical issues. Particularly, iPSCs can be differentiated into any tissue of the human body, following several protocols which use different stimuli to induce specific differentiation processes. Differentiated cells also maintain the genetic heritage of the donor, and therefore are suitable for personalized pharmacological studies; moreover, iPSC-derived differentiated cells are a valuable tool for the investigation of the mechanisms underlying the physiological differentiation processes. iPSCs-derived organoids represent another important tool for the study of ADRs. Precisely, organoids are in vitro 3D models which better represent the native organ, both from a structural and a functional point of view. Moreover, in the same way as iPSC-derived 2D models, iPSC-derived organoids are appropriate personalized models since they retain the genetic heritage of the donor. In comparison to other in vitro models, iPSC-derived organoids present advantages in terms of versatility, patient-specificity, and ethical issues. This review aims to provide an updated report of the employment of iPSCs, and 2D and 3D models derived from these, for the study of ADRs. This article is categorized under: Cancer > Stem Cells and Development.

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iPSC作为研究药物不良反应的开创性工具:个性化治疗的新途径。
通过对不同的体细胞类型进行重新编程获得的诱导多能干细胞(iPSC)是研究药物毒性的一种很有前途的工具,尤其是在个性化医学的背景下。事实上,这些细胞保留了捐赠者相同的遗传遗产,从而可以开发个性化的模型。此外,它们是研究特殊人群药物不良反应(ADR)的有用工具,如儿科患者,由于伦理问题,这些患者在临床试验中的代表性往往很差。特别地,iPSC可以分化为人体的任何组织,遵循几种使用不同刺激来诱导特定分化过程的方案。分化细胞还保持供体的遗传遗产,因此适合进行个性化的药理学研究;此外,iPSC衍生的分化细胞是研究生理分化过程机制的有价值的工具。iPSC衍生的类器官是研究ADR的另一个重要工具。确切地说,类器官是体外3D模型,从结构和功能的角度来看,它更好地代表了天然器官。此外,与iPSC衍生的2D模型相同,iPSC衍生类器官是合适的个性化模型,因为它们保留了供体的遗传遗产。与其他体外模型相比,iPSC衍生的类器官在多功能性、患者特异性和伦理问题方面具有优势。本综述旨在提供一份关于iPSC使用情况的最新报告,以及由此衍生的2D和3D模型,用于ADR研究。本文分类为:癌症>干细胞与发育。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
WIREs Mechanisms of Disease
WIREs Mechanisms of Disease MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
11.40
自引率
0.00%
发文量
45
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